A Study of the Interaction Between trans -Dehydrocrotonin, a Bioactive Natural 19- nor -Clerodane, and Serum Albumin

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The interaction between four antiparasitic drugs (benznidazole (BZL), metronidazole (MTZ), nifurtimox (NFX) and megazol (MZ)) with human serum albumin (HSA), the main vehicle of biodistribution of xenobiotics, hydrophobic, small and endogenous molecules in the bloodstream, was evaluated by multiple spectroscopic techniques and theoretical calculations. In all cases quenching of the fluorescence of HSA by these drugs involve a static mechanism, due to ground state association. There is just one main binding site in HSA for these four ligands (Sudlow's site I); binding is spontaneous, moderate, does not have any effect on the polarity around the Tyr and Trp residues and does not perturb significantly the secondary structure of the protein. Molecular docking studies suggest hydrogen bonding and hydrophobic interactions as the main binding forces, i.e., BZL associates with the Trp-214 residue via hydrophobic interactions and with Gln-220, Arg-221 and Glu-449 residues via hydrogen bonding; whereas MTZ associates with Leu-197 and Leu-480 residues via hydrophobic interactions and with Trp-214, Glu-449 and Ser-453 via hydrogen bonding. Furthermore, electrostatic interactions were also suggested for HSA:MZ and HSA:NFX.

Section: Resultsmentioning

confidence: 99%

Multiple Spectroscopic and Theoretical Approaches to Study the Interaction between HSA and the Antiparasitic Drugs: Benznidazole, Metronidazole, Nifurtimox and Megazol

Chaves¹,

Ferreira²,

Silva³

et al. 2018

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“…1.0 at 296, 303 and 310 K) indicate the existence of just one main binding site in the BSA structure for PIA. 30 Basically, four main types of interaction (hydrogen bond, electrostatic, van der Waals and hydrophobic forces) play critical roles in the association between small molecules and macromolecules. In order to characterize the forces between PIA and BSA, thermodynamic parameters were calculated using the van't Hoff equation (5) where, ΔH°, ΔS°, ΔG° are the enthalpy, entropy and Gibbs free energy change, respectively; R is the gas constant (R = 8.314 × 10 -3 kJ mol -1 K -1 ), T is the temperature (296, 303 and 310 K) and K b the binding constant.…”

Section: Fluorescence Quenching Studiesmentioning

confidence: 99%

“…phenylbutazone, azapropazone, tolbutamide, bucolome and sulfisoxazole), whose structural characteristics are similar to those in the PIA structure. 30,42 Figure 7A represents the molecular surface of BSA for the PIA pose with the best docking score. This figure shows that the major part of the PIA structure is accommodated inside the protein binding site, which could be related to the high binding constants values obtained in the fluorescence quenching experiments.…”

Section: Molecular Dockingmentioning

confidence: 99%

Studies of the Interaction between BSA and a Plumeran Indole Alkaloid Isolated from the Stem Bark of Aspidosperma cylindrocarpon (Apocynaceae)

Chaves¹,

Teixeira²,

Guimarães³

et al. 2016

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Binding between bovine serum albumin (BSA) and a plumeran indole alkaloid (PIA) isolated from the stem bark of Aspidosperma cylindrocarpon (Apocynaceae) was studied by spectroscopic techniques (UV-Vis absorption, circular dichroism, steady state and time-resolved fluorescence), combined with molecular docking. Steady state and time resolved fluorescence data revealed that PIA can quench the BSA fluorescence via a static mechanism: energy transfer from BSA to PIA occurs with high probability. The binding is strong (K b ca. 10 5 -10 6 L mol -1 ), spontaneous (ΔG° ca. -35.7 kJ mol -1 at 310 K) and entropy-driven (ΔS° = 0.146 kJ mol -1 K -1 ). There is just one main binding site (n ca. 1) for the BSA:PIA interaction and the α-helix content of the albumin does not suffer significant perturbation upon PIA binding. Molecular docking results suggest site I as the main binding site to PIA, which is able to interact with the Trp-212, Arg-217, Val-342 and Pro-446 residues.

“…In vitro studies have shown that t-DCTN presents potential effects as antigenotoxic, 6 antileishmanial, 7 antiulcerogenic, 8 antitumor, [9][10][11] and hypoglycemic. 12 Recent publication from our group 13 on the interaction between t-DCTN and bovine serum albumin (BSA) demonstrated that there is a spontaneous, weak and entropy-driven association between BSA and t-DCTN in the ground state, typical of hydrophobic interactions. There is just one main binding site in serum albumin for t-DCTN causing a moderate change in the α-helix content of the albumin.…”

Section: Introductionmentioning

confidence: 99%

“…There is just one main binding site in serum albumin for t-DCTN causing a moderate change in the α-helix content of the albumin. 13 Recently, five semi-synthetic clerodanes based on the t-DCTN structure were synthesized and assayed against Ehrlich carcinoma and K562 human leukemia cells. Two of them showed remarkable biological activity: methyl-hydrazone (MHDCTN, Figure 1) and phenylhydrazone derivative (PHDCTN, Figure 1) 14 Since the binding ability HSA:drug is one of the steps for a possible pharmacological application and considering that MHDCTN and PHDCTN showed potential anti-cancer activity, the aim of the present study is the continuation of investigation of pharmacological aspects through their interaction with HSA.…”

Section: Introductionmentioning

confidence: 99%

In vitro Analysis of the Interaction between Human Serum Albumin and Semi‑Synthetic Clerodanes

Chaves¹,

Echevarrı́a²,

Esteves-Souza³

et al. 2018

The interaction between HSA and two semi-synthetic potential anti-cancer agents derived from trans-dehydrocrotonin-methyl-hydrazone (MHDCTN) and phenyl-hydrazone (PHDCTN) was evaluated under physiological conditions at 296, 303 and 310 K by multi-spectroscopic techniques and molecular docking calculations. Steady state fluorescence quenching indicated a ground state association (static quenching) for both samples; however, the quenching induced by PHDCTN was not essentially static and can be accompanied by a dynamic quenching mechanism. The binding is strong (modified Stern-Volmer binding constant (K a ) ca. 10 5 M -1 ), causing a very weak perturbation on the secondary structure of the protein and there is just one main binding site for both samples (Sudlow's site I). Molecular docking results suggested hydrogen bonding and hydrophobic interactions as the main binding forces for both samples.